Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need

Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need

To date, reperfusion with tissue plasminogen activator (tPA) remains the gold standard treatment for ischemic stroke. However, when tPA is given beyond 4.5 hours of stroke onset, deleterious effects of the drug ensue, especially, hemorrhagic transformation (HT), which causes the most significant mor...

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Main Authors: Ike dela Peña, Cesar Borlongan, Guofang Shen, Willie Davis
Format: Article
Language:English
Published: Korean Stroke Society 2017-01-01
Series:Journal of Stroke
Subjects:
tissue plasminogen activator
hemorrhage
vasculature
blood-brain barrier
Online Access:http://www.j-stroke.org/upload/pdf/jos-2016-01515.pdf
id doaj-f5b9a89b95834718b472665c8c842847
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spelling doaj-f5b9a89b95834718b472665c8c8428472020-11-25T02:20:41ZengKorean Stroke SocietyJournal of Stroke2287-63912287-64052017-01-01191506010.5853/jos.2016.01515166Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical NeedIke dela Peña0Cesar Borlongan1Guofang Shen2Willie Davis3 Department of Pharmaceutical and Administrative Sciences, Loma Linda University School of Pharmacy, Loma Linda, United States Center of Excellence for Aging and Brain Repair, Department of Neurosurgery and Brain Repair, University of South Florida Morsani College of Medicine, Tampa, United States Department of Pharmaceutical and Administrative Sciences, Loma Linda University School of Pharmacy, Loma Linda, United States Department of Pharmaceutical and Administrative Sciences, Loma Linda University School of Pharmacy, Loma Linda, United StatesTo date, reperfusion with tissue plasminogen activator (tPA) remains the gold standard treatment for ischemic stroke. However, when tPA is given beyond 4.5 hours of stroke onset, deleterious effects of the drug ensue, especially, hemorrhagic transformation (HT), which causes the most significant morbidity and mortality in stroke patients. An important clinical problem at hand is to develop strategies that will enhance the therapeutic time window for tPA therapy and reduce the adverse effects (especially HT) of delayed tPA treatment. We reviewed the pharmacological agents which reduced the risk of HT associated with delayed (beyond 4.5 hours post-stroke) tPA treatment in preclinical studies, which we classified into those that putatively preserve the blood-brain barrier (e.g., minocycline, cilostazol, fasudil, candesartan, and bryostatin) and/or enhance vascularization and protect the cerebrovasculature (e.g., coumarin derivate IMM-H004 and granulocyte colony-stimulating factor). Recently, other new therapeutic modalities (e.g., oxygen transporters) have been reported which improved delayed tPA-associated outcomes by acting through other mechanisms. While the above-mentioned interventions unequivocally reduced delayed tPA-induced HT in stroke models, the long-term efficacy of these drugs are not yet established. Further optimization is required to expedite their future clinical application. The findings from this review indicate the need to explore the most ideal adjunctive interventions that will not only reduce delayed tPA–induced HT, but also preserve neurovascular functions. While waiting for the next breakthrough drug in acute stroke treatment, it is equally important to allocate considerable effort to find approaches to address the limitations of the only FDA-approved stroke therapy.http://www.j-stroke.org/upload/pdf/jos-2016-01515.pdftissue plasminogen activatorhemorrhagevasculatureblood-brain barrier
collection DOAJ
language English
format Article
sources DOAJ
author Ike dela Peña
Cesar Borlongan
Guofang Shen
Willie Davis
spellingShingle Ike dela Peña
Cesar Borlongan
Guofang Shen
Willie Davis
Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need
Journal of Stroke
tissue plasminogen activator
hemorrhage
vasculature
blood-brain barrier
author_facet Ike dela Peña
Cesar Borlongan
Guofang Shen
Willie Davis
author_sort Ike dela Peña
title Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need
title_short Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need
title_full Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need
title_fullStr Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need
title_full_unstemmed Strategies to Extend Thrombolytic Time Window for Ischemic Stroke Treatment: An Unmet Clinical Need
title_sort strategies to extend thrombolytic time window for ischemic stroke treatment: an unmet clinical need
publisher Korean Stroke Society
series Journal of Stroke
issn 2287-6391
2287-6405
publishDate 2017-01-01
description To date, reperfusion with tissue plasminogen activator (tPA) remains the gold standard treatment for ischemic stroke. However, when tPA is given beyond 4.5 hours of stroke onset, deleterious effects of the drug ensue, especially, hemorrhagic transformation (HT), which causes the most significant morbidity and mortality in stroke patients. An important clinical problem at hand is to develop strategies that will enhance the therapeutic time window for tPA therapy and reduce the adverse effects (especially HT) of delayed tPA treatment. We reviewed the pharmacological agents which reduced the risk of HT associated with delayed (beyond 4.5 hours post-stroke) tPA treatment in preclinical studies, which we classified into those that putatively preserve the blood-brain barrier (e.g., minocycline, cilostazol, fasudil, candesartan, and bryostatin) and/or enhance vascularization and protect the cerebrovasculature (e.g., coumarin derivate IMM-H004 and granulocyte colony-stimulating factor). Recently, other new therapeutic modalities (e.g., oxygen transporters) have been reported which improved delayed tPA-associated outcomes by acting through other mechanisms. While the above-mentioned interventions unequivocally reduced delayed tPA-induced HT in stroke models, the long-term efficacy of these drugs are not yet established. Further optimization is required to expedite their future clinical application. The findings from this review indicate the need to explore the most ideal adjunctive interventions that will not only reduce delayed tPA–induced HT, but also preserve neurovascular functions. While waiting for the next breakthrough drug in acute stroke treatment, it is equally important to allocate considerable effort to find approaches to address the limitations of the only FDA-approved stroke therapy.
topic tissue plasminogen activator
hemorrhage
vasculature
blood-brain barrier
url http://www.j-stroke.org/upload/pdf/jos-2016-01515.pdf
work_keys_str_mv AT ikedelapena strategiestoextendthrombolytictimewindowforischemicstroketreatmentanunmetclinicalneed
AT cesarborlongan strategiestoextendthrombolytictimewindowforischemicstroketreatmentanunmetclinicalneed
AT guofangshen strategiestoextendthrombolytictimewindowforischemicstroketreatmentanunmetclinicalneed
AT williedavis strategiestoextendthrombolytictimewindowforischemicstroketreatmentanunmetclinicalneed
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